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For Healthcare Professionals

Safety

SAFETY

WITHIN 1 YEAR FOLLOWING TREATMENT, LENMELDY WAS GENERALLY WELL TOLERATED1

Non-laboratory, treatment-emergent adverse reactions reported in ≥10% of patients within year 1 following treatment with LENMELDY (N=39)*

  • In clinical trials, 11 patients (28%) developed an adverse reaction of neutropenia following conditioning, 8 of whom (21%) experienced a Grade 3 event
  • 3 patients (8%) developed an adverse reaction of anemia, 1 of whom experienced a Grade 3 event
  • 9 patients (23%) developed elevated liver enzymes, including 3 patients (8%) who developed a Grade 3 event
  • Elevated levels of D-dimer (greater than 4.2 nmol/L) have been reported in 26/39 (67%) patients during clinical trials of LENMELDY. Abnormal values up to 109.5 nmol/L were identified at timepoints from day 21 to year 7 after LENMELDY infusion, with no pattern identified

Events that occurred in <10% of the population included:

  • 1 patient experienced Grade 3 adverse reactions of elevated alanine and aspartate transaminases that met the definition of Hy’s Law at day 14 after LENMELDY infusion and resolved without treatment by 9 months after initial onset
  • 2 patients experienced Grade 3 elevations in liver enzymes, and 1 patient experienced Grade 1 elevations in liver enzymes
  • All events resolved without treatment and are considered related to conditioning
* Includes adverse events potentially related to busulfan myeloablative conditioning.
a Includes events with preferred terms (PTs) of bronchitis, nasopharyngitis, pharyngitis, pneumonia, respiratory tract infection, rhinitis, tonsillitis, upper respiratory fungal infection, and upper respiratory tract infection.
b Includes events of bacterial sepsis, catheter site cellulitis, catheter site infection, device-related infection, sepsis, and vascular device infection.
c Includes events with PTs of enteritis, gastroenteritis, gastroenteritis aeromonas, and gastroenteritis rotavirus.
d Includes events with PTs of adenovirus infection, cytomegalovirus infection, cytomegalovirus test positive, cytomegalovirus viremia, enterovirus infection,
hand-foot-and-mouth disease, herpes zoster, SARSCov-2-test positive, and viral infection (excluding PT of gastroenteritis rotavirus).
e Includes events with PTs of dermatitis, dermatitis bullous, rash, rash erythematous, drug eruption, and rash maculopapular.

Reference: 1. LENMELDY (atidarsagene autotemcel) Prescribing Information. Orchard Therapeutics.

IMPORTANT SAFETY INFORMATION

WARNINGS AND PRECAUTIONS

• Thrombosis and Thromboembolic Events:

Treatment with LENMELDY may increase the risk of thrombosis and thromboembolic events.

INDICATION

LENMELDY™ (atidarsagene autotemcel) is an autologous hematopoietic stem cell-based gene therapy indicated for the treatment of children with pre-symptomatic late infantile (PSLI), pre-symptomatic early juvenile (PSEJ), or early symptomatic early juvenile (ESEJ) metachromatic leukodystrophy (MLD).

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